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Characterization of apoptosis in a motor neuron cell line.

机译:运动神经元细胞系中凋亡的表征。

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STUDY DESIGN: Serum withdrawal was introduced to a spinal cord motor neuron cell line to investigate the mode of cell death. OBJECTIVES: To characterize the death of motor neurons in culture, to gain insight into mechanisms that could be important in spinal cord diseases. SUMMARY OF BACKGROUND DATA: Normal reduction of cell number during central nervous system development is brought about by programmed cell death. These same apoptotic processes probably play a role in a variety of central nervous system disorders, including traumatic injury. Although certain proteolytic processes are involved, the molecular details involved in the apoptotic induction have not been fully elucidated. METHODS: To identify apoptosis, several criteria were used, including analysis of chromatin condensation with DNA-specific stains (propidium iodide and Hoechst 33342); in situ end-labeling of DNA fragments in apoptotic nuclei with terminal deoxynucleotidyl transferase; fragmentation of DNA separated on agarose gel electrophoresis; and cleavage of a characteristic substrate for apoptotic proteases, alpha-fodrin, into signature cleavage fragments. RESULTS: The NSC19 cell line exhibited motor neuron characteristics morphologically, with typical cellular structure, and biochemically, by synthesizing choline acetyl transferase. Under various treatments including serum withdrawal (loss of trophic factors), cell loss occurred through an apoptotic cell death pathway. CONCLUSIONS: A murine motor neuron cell line, NSC19, has been used to investigate apoptosis in this in vitro system. Cell death occurs by apoptosis, suggesting that this cell line may provide a useful model for studying apoptotic mechanisms in spinal cord degeneration and injury.
机译:研究设计:将血清戒断引入脊髓运动神经元细胞系,以研究细胞死亡的方式。目的:表征培养物中运动神经元的死亡,深入了解可能对脊髓疾病重要的机制。背景数据概述:中枢神经系统发育过程中正常数量的细胞减少是由程序性细胞死亡引起的。这些相同的凋亡过程可能在包括创伤性损伤在内的多种中枢神经系统疾病中起作用。尽管涉及某些蛋白水解过程,但尚未完全阐明凋亡诱导中涉及的分子细节。方法:为了鉴定细胞凋亡,使用了一些标准,包括用DNA特异性染料(碘化丙啶和Hoechst 33342)分析染色质浓缩。用末端脱氧核苷酸转移酶原位末端标记凋亡核中的DNA片段;琼脂糖凝胶电泳分离的DNA片段;将凋亡蛋白酶的特征底物α-fodrin裂解为标志性裂解片段。结果:通过合成胆碱乙酰基转移酶,NSC19细胞系表现出运动神经元特征,具有典型的细胞结构和生化特征。在包括血清停药(营养因子丧失)在内的各种治疗下,细胞凋亡是通过凋亡性细胞死亡途径发生的。结论:鼠运动神经元细胞系NSC19已用于研究该体外系统的细胞凋亡。细胞死亡是通过凋亡发生的,这表明该细胞系可能为研究脊髓变性和损伤中的凋亡机制提供有用的模型。

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